Borosky Gabriela L, Laali Kenneth K
Unidad de Matematica y Física, INFIQC, Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, Ciudad Universitaria, Argentina.
Chem Res Toxicol. 2006 Jul;19(7):899-907. doi: 10.1021/tx060067l.
Structure-reactivity relationships and substituent effects on carbocation stability in benzo[a]anthracene (BA) derivatives have been studied computationally at the B3LYP/6-31G and MP2/6-31G levels. Bay-region carbocations are formed by O-protonation of the 1,2-epoxides in barrierless processes. This process is energetically more favored as compared to carbocation generation via zwitterion formation/O-protonation, via single electron oxidation to generate a radical cation, or via benzylic hydroxylation. Relative carbocation stabilities were determined in the gas phase and in water as solvent (PCM method). Charge delocalization mode in the BA carbocation framework was deduced from NPA-derived changes in charges, and substitution by methyl or fluorine was studied at different positions selected on basis of the carbocation charge density. A bay-region methyl group produces structural distortion with consequent deviation from planarity of the aromatic system, which destabilizes the epoxide, favoring ring opening. Whereas fluorine substitution at sites bearing significant positive charge leads to carbocation stabilization by fluorine p-pi back-bonding, a fluorine atom at a ring position which presented negative charge density leads to inductive destabilization. Methylated derivatives are less sensitive to substituent effects as compared to the fluorinated analogues. Although the solvent decreases the exothermicity of the epoxide ring-opening reactions due to greater stabilization of the reactants, it provokes no changes in relative reactivities. Relative energies in the resulting bay-region carbocations are examined taking into account the available biological activity data on these compounds. In selected cases, quenching of bay-region carbocations was investigated by analyzing relative energies (in the gas phase and in water) and geometries of their guanine adducts formed via covalent bond formation with the exocyclic amino group and with the N-7.
在B3LYP/6 - 31G和MP2/6 - 31G水平上,通过计算研究了苯并[a]蒽(BA)衍生物中结构 - 反应性关系以及取代基对碳正离子稳定性的影响。湾区碳正离子是通过1,2 - 环氧化物的O - 质子化在无势垒过程中形成的。与通过两性离子形成/O - 质子化、通过单电子氧化生成自由基阳离子或通过苄基羟基化生成碳正离子相比,这个过程在能量上更有利。在气相和以水为溶剂(PCM方法)的条件下测定了相对碳正离子稳定性。从NPA衍生的电荷变化推导出BA碳正离子骨架中的电荷离域模式,并根据碳正离子电荷密度在不同位置研究了甲基或氟的取代情况。湾区甲基会产生结构畸变,导致芳香体系偏离平面性,使环氧化物不稳定,有利于开环。而在带有显著正电荷的位点进行氟取代会通过氟的p - π反馈键合使碳正离子稳定,在呈现负电荷密度的环位置上的氟原子会导致诱导失稳。与氟化类似物相比,甲基化衍生物对取代基效应不太敏感。尽管溶剂由于反应物的更稳定化而降低了环氧化物开环反应的放热性,但它不会引起相对反应性的变化。考虑到这些化合物现有的生物活性数据,研究了所得湾区碳正离子的相对能量。在选定的情况下,通过分析相对能量(在气相和水中)以及它们通过与环外氨基和N - 7形成共价键而形成的鸟嘌呤加合物的几何结构,研究了湾区碳正离子的猝灭情况。